RT Journal Article
SR Electronic
T1 Absorbed Fractions for α-Particles in Tissues of Trabecular Bone: Considerations of Marrow Cellularity Within the ICRP Reference Male
JF Journal of Nuclear Medicine
JO J Nucl Med
FD Society of Nuclear Medicine
SP 1171
OP 1185
VO 46
IS 7
A1 Watchman, Christopher J.
A1 Jokisch, Derek W.
A1 Patton, Phillip W.
A1 Rajon, Didier A.
A1 Sgouros, George
A1 Bolch, Wesley E.
YR 2005
UL http://jnm.snmjournals.org/content/46/7/1171.abstract
AB α-Particles are of current interest in radionuclide therapy due to their short range and high rates of energy transfer to target tissues. Published values of α-particle absorbed fraction φ in the skeletal tissues, as needed for patient-specific dosimetry under the MIRD schema, do not generally account for its variation with particle energy or skeletal site. Furthermore, variations in α-particle absorbed fraction with marrow cellularity have yet to be fully considered. Methods: In this study, a 3-dimensional (3D) chord-based radiation transport model (or 3D-CBIST) is presented, which combines (a) chord-based techniques for tracking α-particles across bone trabeculae, endosteum, and marrow cavities and (b) a spatial model of the marrow tissues that explicitly considers the presence of marrow adipocytes. Chord-length distributions are taken from a 44-y male subject (ICRP [International Commission on Radiological Protection] Reference Male) and are identical to those used currently for clinical dose estimates for β-particle emitters. Results: Values of φ(active marrow←active marrow) given by the 3D-CBIST model are shown to be considerably lower than φ = 1.0 assumed under the ICRP Publication 30 and 2003 Eckerman bone models. For example, values of absorbed fraction for the self-dose to active bone marrow in the ribs, cervical vertebra, and parietal bone are 0.81, 0.80, and 0.55 for 6-MeV α-particles and are 0.74, 0.72, and 0.43 for 9-MeV α-particles, where each is evaluated at ICRP reference cellularities in the 3D-CBIST model (72%, 72%, and 42%, respectively, at age 25 y). Conclusion: Improvements in patient-specific dosimetry of skeletal tissues require explicit consideration of not only changes in target mass with variable patient marrow cellularity (i.e., active marrow) but also corresponding changes in values of the absorbed fraction. The data given in this study provide a more-firm basis for application of the MIRD schema to patient-specific dosimetry for newly developing therapies using α-particle emitters.